Effect of amitraz and its metabolites on intestinal motility
1. Amitraz was rapidly metabolised to BTS27271 after intravenous administration to sheep. 2. Amitraz and BTS27271 had significant H1-histamine antagonist activity on isolated guinea-pig ileum. BTS27271 was approximately 3.3 times as potent as amitraz. 3. Intravenous injection of amitraz and its meta...
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| Published in: | Comparative biochemistry and physiology. C, Comparative pharmacology and toxicology Vol. 99; no. 1-2; p. 169 |
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| Main Authors: | , |
| Format: | Journal Article |
| Language: | English |
| Published: |
England
1991
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| Abstract | 1. Amitraz was rapidly metabolised to BTS27271 after intravenous administration to sheep. 2. Amitraz and BTS27271 had significant H1-histamine antagonist activity on isolated guinea-pig ileum. BTS27271 was approximately 3.3 times as potent as amitraz. 3. Intravenous injection of amitraz and its metabolite BTS27271 caused an immediate cessation of caecal motility in sheep, which persisted for 74-245 min. 4. Caecal stasis induced by amitraz was reversed by yohimbine but only partially reversed by 2-pyridylethylamine. 5. The results suggest that despite the significant antihistamine activity of amitraz and BTS27271 in vitro, it is probably the alpha-2-adrenergic agonist activity that is the most important in causing large intestinal stasis in vivo. |
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| AbstractList | 1. Amitraz was rapidly metabolised to BTS27271 after intravenous administration to sheep. 2. Amitraz and BTS27271 had significant H1-histamine antagonist activity on isolated guinea-pig ileum. BTS27271 was approximately 3.3 times as potent as amitraz. 3. Intravenous injection of amitraz and its metabolite BTS27271 caused an immediate cessation of caecal motility in sheep, which persisted for 74-245 min. 4. Caecal stasis induced by amitraz was reversed by yohimbine but only partially reversed by 2-pyridylethylamine. 5. The results suggest that despite the significant antihistamine activity of amitraz and BTS27271 in vitro, it is probably the alpha-2-adrenergic agonist activity that is the most important in causing large intestinal stasis in vivo. |
| Author | Mogg, T D Pass, M A |
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| Snippet | 1. Amitraz was rapidly metabolised to BTS27271 after intravenous administration to sheep. 2. Amitraz and BTS27271 had significant H1-histamine antagonist... |
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| SubjectTerms | Amidines - pharmacology Animals Cecum - drug effects Cecum - physiology Chromatography, High Pressure Liquid Female Gastrointestinal Motility - drug effects Guinea Pigs Ileum - drug effects Ileum - physiology Insecticides - metabolism Insecticides - pharmacology Kinetics Muscle Contraction - drug effects Pyridines - pharmacology Sheep Toluidines - metabolism Toluidines - pharmacology Yohimbine - pharmacology |
| Title | Effect of amitraz and its metabolites on intestinal motility |
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